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B淋巴细胞中的免疫球蛋白(Ig)同种型转换。T细胞衍生的白细胞介素、细胞因子、霍乱毒素和抗原对克隆的B细胞淋巴瘤同种型转换频率的影响。

Ig isotype switching in B lymphocytes. The effect of T cell-derived interleukins, cytokines, cholera toxin, and antigen on isotype switch frequency of a cloned B cell lymphoma.

作者信息

Whitmore A C, Prowse D M, Haughton G, Arnold L W

机构信息

Department of Microbiology and Immunology, University of North Carolina, Chapel Hill 27599.

出版信息

Int Immunol. 1991 Jan;3(1):95-103. doi: 10.1093/intimm/3.1.95.

DOI:10.1093/intimm/3.1.95
PMID:2049338
Abstract

The murine B cell lymphoma CH12.LX, which bears cell surface IgM specific for the phosphatidyl choline epitope of sheep red blood cells, is capable of spontaneous isotype switching in vitro. Switching to IgG3, IgG1, IgG2b, and IgA has been observed and variants expressing those isotypes have been isolated and cloned. We have developed a procedure for precise numerical evaluation of the frequency of switching to the several isotypes to which CH12.LX can switch. We have used a modified Poisson method which can distinguish between treatments which change isotype switch frequency and those which affect, in an isotype-specific fashion, growth or secretion rates of cells which have already switched. In this report we examine the effect of several cytokines, cholera toxin, hydroxyurea, and antigen on the isotype switch frequency of CH12.LX. The strongest effect observed was that of transforming growth factor-beta, which increases switch frequency 40-fold to an absolute switch frequency of 0.04 switch events (from IgM to IgA expression) per cell division. Interleukin-4 (IL-4) and cholera toxin also increase the switch frequency of CH12.LX while IL-5, IL-6 (with or without antigen), antigen (SRBC) alone, interferon-gamma, or hydroxyurea have no effect. We have shown that none of the cytokines studied change the relative frequency of switching to the available isotypes, only the absolute frequency of switching. We infer from this that the factors tested do not 'instruct' CH12.LX to switch to a particular isotype, but rather they deliver a 'go' signal to cells committed to switching to IgA at high frequency, rarely to IgG3, IgG1, or IgG2b, and never to IgG2a or IgE.

摘要

鼠源B细胞淋巴瘤CH12.LX细胞表面带有针对绵羊红细胞磷脂酰胆碱表位的IgM,能够在体外自发进行同种型转换。已观察到向IgG3、IgG1、IgG2b和IgA的转换,并且分离和克隆了表达这些同种型的变体。我们开发了一种程序,用于精确数值评估CH12.LX可转换的几种同种型的转换频率。我们使用了一种改良的泊松方法,该方法可以区分改变同种型转换频率的处理和以同种型特异性方式影响已转换细胞生长或分泌速率的处理。在本报告中,我们研究了几种细胞因子、霍乱毒素、羟基脲和抗原对CH12.LX同种型转换频率的影响。观察到的最强效应是转化生长因子-β的效应,它将转换频率提高了40倍,达到每细胞分裂0.04次转换事件(从IgM表达转换为IgA表达)的绝对转换频率。白细胞介素-4(IL-4)和霍乱毒素也增加了CH12.LX的转换频率,而IL-5、IL-6(有无抗原)、单独的抗原(SRBC)、干扰素-γ或羟基脲则没有影响。我们已经表明,所研究的细胞因子均未改变转换到可用同种型的相对频率,只是改变了转换的绝对频率。由此我们推断,所测试的因子不会“指导”CH12.LX转换到特定的同种型,而是向致力于高频转换到IgA的细胞发出“启动”信号,很少向IgG3、IgG1或IgG2b发出信号,从不向IgG2a或IgE发出信号。

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